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A Functional Variant at miR-520a Binding Site in PIK3CA Alters Susceptibility to Colorectal Cancer in a Chinese Han Population

机译:MIR-520A粘结位点的官能变体在PIK3CA中改变了中国汉族人群的直肠癌的易感性

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An increasing body of evidence has indicated that polymorphisms in the miRNA binding site of target gene can alter the ability of miRNAs to bind their target genes and modulate the risk of cancer. We aimed to investigate the association between a miR-520a binding site polymorphism rsl41178472 in the PIK3CA 3'-UTR and the risk of colorectal cancer (CRC) in a Chinese Han population. The polymorphism rsl41178472 was analyzed in a case-control study, including 386 CRC patients and 394 age- and sex-matched controls; the relationship between the polymorphism and the risk of colorectal cancer was examined. Individuals carrying the rsl41178472 CC genotype or C allele had an increased risk of developing CRC (CC versus TT, OR (95% CI): 1.716 (1.084-2.716), P = 0.022; C versus T, OR (95% CI): 1.258 (1.021-1.551), P - 0.033). Furthermore, the expression of PIK3CA was detected in the peripheral blood mononudeated cell of CRC patients, suggesting that mRNA levels of PIK3CA might be associated with SNP rsl41178472. These findings provide evidence that a miR-520a binding site polymorphism rsl41178472 in the PIK3CA 3'-UTR may play a role in the etiology of CRC.
机译:越来越多的证据表明,靶基因的miRNA结合位点中的多态性可以改变miRNA结合其靶基因并调节癌症风险的能力。我们旨在探讨MIR-520A结合位点多态性RSL41178472在PIK3CA 3'-UTR中的关联以及中国汉族人群中结肠直肠癌(CRC)的风险。在病例对照研究中分析多态RSL41178472,包括386例CRC患者和394名年龄和性别匹配的对照;检查了多态性与结直肠癌风险的关系。携带RSL41178472 CC基因型或C等位基因的个体具有增加的开发CRC的风险(CC与TT,或(95%CI):1.716(1.084-2.716),P = 0.022; C与T,或(95%CI): 1.258(1.021-1.551),P - 0.033)。此外,在CRC患者的外周血单血细胞中检测到PIK3CA的表达,表明PIK3CA的mRNA水平可能与SNP RSL41178472相关。这些发现提供了证据表明,PIK3CA 3'-UTR中的miR-520A结合位点多态性RSL41178472可以在CRC的病因中起作用。

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